Breast Pathology News, WHO Update · Breast Pathology News, WHO Update Emad Rakha Professor of...
Transcript of Breast Pathology News, WHO Update · Breast Pathology News, WHO Update Emad Rakha Professor of...
Breast Pathology News, WHO
Update
Emad Rakha
Professor of Breast Pathology School of Medicine, University of Nottingham
Permission from Ian Cree (Head, WHO classification of tumours group is obtained)
Foreword• The most conspicuous change to the format of the books in the fifth edition is
that tumour types common to multiple systems are dealt with together – so there are separate chapters on haematolymphoid tumours and mesenchymal tumours. There is also a chapter on genetic tumour syndromes..…
• We have attempted to take a more systematic approach to the multifaceted nature of tumour classification; each tumour type is described on the basis of its localization, clinical features, epidemiology, etiology, pathogenesis, histopathology, diagnostic molecular pathology, staging, and prognosis and prediction.
• We have also included information on macroscopic appearance and cytology, as well as essential and desirable diagnostic criteria. This standardized, modular approach makes it easier for the books to be accessible online, but it also enables us to call attention to areas in which there is little information, and where serious gaps in our knowledge remain to be addressed.
• The organization of the WHO Blue Books content now follows the normal progression from benign to malignant – a break with the fourth edition, but one we hope will be welcome.
Dr Ian A. Cree, Head, WHO Classification of Tumours Group, International Agency for Research on Cancer, August 2019
5th edition of the WHO book2019
2.7.4: Tubular carcinoma
Definition
Related terminology
Subtype(s)
Localization
Clinical features
Epidemiology
Etiology
Pathogenesis
Macroscopic appearance
Histopathology
Cytology
Diagnostic molecular pathology
Essential and desirable diagnostic criteria
Staging
Prognosis and prediction
References:
Microinvasive carcinoma
• Some earlier definitions mandated that invasion should be present into the non-specialized stroma, but this is no longer a requirement
• The distinction between specialized stroma and the non-specialized (interlobular) stroma can generally be made in normal breast histology but becomes less obvious when an inflammatory infiltrate and oedema obscure the boundary
• Defined as: Invasion beyond the myoepithelium and the basement membrane of the in situ component (≤1mm)
• Sometimes also lower grade DCIS, lobular carcinoma in situ (LCIS) or Paget’s disease of the nipple
5th edition of the WHO book
Some rare special typesSpecial morphologic patterns of NST:
• Oncocytic
• Lipid rich,
• Glycogen rich
• Clear cell
• Sebaceous carcinomas
• Similarly, invasive carcinoma with neuroendocrine differentiation, pleomorphic and choriocarcinomatous pattern and tumours with melanocytic features
• Rare tumours with no sufficient clinical evidence available for their designation as special tumour subtypes and their specific pattern is considered as part of the spectrum of differentiation seen in the IBC, NST.
• Considered as morphological patterns of IBC, NST regardless of the extent of differentiation/ pattern and the 90% role for special subtype is not applied to tumours showing any of these patterns
5th edition of the WHO book
Medullary Carcinoma• Described as a special type of BC with high grade
features but with good prognosis• Sharply circumscribed soft, rounded tumour mass
with pushing rather than infiltrating margin• Interconnecting sheets of large, bizarre and
pleomorphic carcinoma cells forming a syncytial network
• Rich in lympho-plasmacytoid cell infiltrates• In situ component insignificant • Typically triple negative• ?Better outcome than grade and stage matched NST
WHO 2012: Carcinomas with medullary features
Definition
Carcinomas with medullary features include
Medullary carcinomas
Atypical medullary carcinomas
A subset of invasive ductal carcinomas of no special type
These tumours demonstrate all or some of the following features:
a circumscribed or pushing border
a syncytial growth pattern
cells with high-grade nuclei
prominent lymphoid infiltration
Medullary Carcinoma
Medullary CarcinomaSpecial morphologic patterns of NST:
"Medullary-like" patterns:
• For clinical purposes, it is now proposed that carcinomas with medullary features are considered one end of the spectrum of the TILs-rich IBC, NST, rather than distinct morphologic subtype.
• These can be described as having histologic features that correlate with the "basal-like" molecular profiles, with some quantification of the degree of TILs present, if clinically relevant.
• However, they are categorized diagnostically as IBC, NST with inclusion of descriptive modifiers referring to medullary-like or basal-like features.
5th edition of the WHO book
Mucinous cystadenocarcinoma• Mucinous cystadenocarcinoma is an invasive breast carcinoma
characterized by cystic structures lined by tall columnar cells with abundant intracytoplasmic mucin, resembling pancreato-biliary or ovarian mucinous cystadenocarcinoma.
• Columnar cells show stratification, tufting, and papillary formations. The neoplastic cells have basally located nuclei and contain abundant intracytoplasmic mucin
5th edition of the WHO book
• A very rare variant of breast carcinoma showing overlapping features between SPC, papillary DCIS, infiltrating epitheliosis and invasive papillary carcinomas
• Circumscribed nests of epithelial cells distributed most often in dense fibrous stroma with a solid papillary pattern. True papillae and cystic structures containing colloid-like material can be observed in some cases
• Nuclear features resembling tall cell variant of PTC in addition to reverse of polarity
• Most triple-negative phenotype, the remaining cases show weak or focal hormone receptor expression
• Express both low and high molecular weight cytokeratins; NE markers are negative; TTF1-ve
• Myoepithelial cells absent or very focal• Most commonly associated with IDH2 R172 hotspot mutations.
Tall cell carcinoma with reversed polarity5th edition of the WHO book
A very rare variant of breast carcinoma, originally designated "breast tumor resembling the tall cell variant of papillary thyroid carcinoma” in 2003 by Eusebi
Different terminology: Solid papillary breast carcinomas resembling the tall cell variant of papillary thyroid neoplasmTall cell variant of papillary breast carcinoma (attempt to avoid confusion with papillary thyroid carcinoma) Solid papillary carcinoma with reverse polarity (SPCRP) (Chiang et al)
5th edition WHO book = Tall cell carcinoma with reversed polarity
Removed words “papillary” or “solid papillary” from name and considered as a variant of invasive carcinoma
Essential and desirable diagnostic criteria
Essential:An invasive breast carcinoma with the neoplastic cell nests arranged in a predominantly solid papillary pattern, composed of columnar epithelial cells showing reverse polarity of the nuclei. Absence of myoepithelial cells around the tumour nests
Desirable:Expression of both low and high molecular weight cytokeratins, and a triple negative or weakly hormone receptor positive phenotype
Staging:Should be staged as invasive breast carcinoma
5th edition of the WHO book
Papillary carcinomas
Neuroendocrine Neoplasms• In the 2012 fourth-edition volume WHO classification of tumours of
the breast, NECs were included under the category “carcinomas with neuroendocrine features”
• Defined as tumours exhibiting morphological features similar to those of NETs of the gastrointestinal tract and lung and expressing neuroendocrine markers to any extent
• NETs in the breast were classified into two main categories:
(1) “NETs, well-differentiated”, which included low- and intermediate-grade tumours
(2) “NECs, poorly differentiated / small cell carcinomas” – these neoplasms, based on the description, included small cell NEC (SCNEC) but not large cell NEC (LCNEC)
This classification also acknowledged the existence of a third category, which comprised a subset of breast carcinomas with neuroendocrine differentiation as determined by histochemical and immunohistochemical analysis; this category included breast carcinoma of no special type (NST), as well as special types such as solid papillary carcinoma and the hypercellular subtype of mucinous carcinoma
Neuroendocrine tumourDefinition
• Neuroendocrine tumour (NET) is an invasive tumour characterized by low/intermediate-grade neuroendocrine morphology, supported by the presence of neurosecretory granules and a diffuse, uniform immunoreactivity for neuroendocrine markers.
Essential and desirable diagnostic criteria
• Essential: histological features and immunoprofilecharacteristic of neuroendocrine differentiation; NETs are not high-grade neoplasms.
• Desirable: coexisting ductal carcinoma in situ.
5th edition of the WHO book
Neuroendocrine carcinomaDefinition
• Neuroendocrine carcinoma (NEC) is an invasive carcinoma characterized by high-grade neuroendocrine morphology (small cell or large cell), supported by the presence of neurosecretory granules and a diffuse, uniform immunoreactivity for neuroendocrine markers
Essential and desirable diagnostic criteria
• Essential: histological features similar to those of SCNEC and LCNEC of the lung; high-grade tumour.
• Desirable: coexisting ductal carcinoma in situ.
5th edition of the WHO book
Neuroendocrine tumours of the breast
Mixed IBC, NST and special subtypes
• If the special subtype makes up between 10-90% of the cancer the terminology mixed IBC, NST and special subtype carcinoma may be used
• For this type of mixed IBC, NST and special subtype, recommended that both elements present be reported and overall percentage of special subtype (example: "Mixed invasive breast carcinoma NST and invasive lobular carcinoma (30% lobular)")
• Grade and biomarker status of both components should be reported, since they can be distinct
5th edition of the WHO book
Subtype(s) of breast carcinomas:
• Invasive breast carcinomas are grouped into the following biomarker-defined subtypes/groups for treatment purposes based on ER and HER2 status as follows:
• ER positive, HER2 negative
• ER positive, HER2 positive
• ER negative, HER2 positive
• ER negative, HER2 negative
• Despite the overlapping morphological features of these biomarker-defined subtypes, they show distinct outcomes and responses to therapy in addition to differences in their global genomic and transcriptomic profiles
Diagnostic molecular pathology:
Molecular classification
Intrinsic subtypes classification
Integrative clusters (IntClust) classification
Triple-negative breast cancer molecular subclassification
Mutation profiles of IBC
5th edition of the WHO book
Tumour-infiltrating lymphocytes (TILs):
The presence and extent of TILs in invasive breast carcinomas are gaining importance as a prognostic marker with high TILs associated with a better outcome and a better response to neoadjuvant therapy in Triple-negative and HER2 positive breast carcinomas
If quantifying TILs, it is recommended to follow the internal consensus scoring recommendations. [International Immuno-Oncology Biomarker Working Group on Breast Cancer; 2018. Available from: https://www.tilsinbreastcancer.org/.]
Main updates
1. Updates of some subheadings such as pathogenesis,
cytology, and essential and desirable diagnostic criteria for
each tumour type
2. Some updates of the classification system and
arrangements of entities
3. Merging some entities: Medullary carcinomas and some
very rare tumour types with NST carcinomas
4. Description of few entities not in the previous edition:
Mucinous cystadenocarcinoma, LCNEC, and introduction of
new entity “tall cell carcinoma with reversed polarity”
5. Update of NE and papillary tumours sections
6. Some updates on the prognostic variables in breast such as
TILs, and molecular features such as mutational profiles,
HER2 guidelines, and biomarker-based subtypes defined
based of ER and HER2